Immunosympathectomy: lack of evidence for a complement-mediated cytotoxic mechanism.
Brain Res
; 201(2): 399-409, 1980 Nov 17.
Article
in En
| MEDLINE
| ID: mdl-6106528
To determine whether the destruction of peripheral sympathetic neurons by anti-NGF-antibodies results from a complement-mediated cytotoxic action or from the deprivation of endogenous NGF or immunologically NGF-like cross-reacting molecules we investigated the time-course of the reversibility of the effect of NGF-antibodies by neutralizing doses of NGF, together with the effect of NGF-antibodies in complement-deficient mice. After administration of a single dose of 50 mg/kg of purified antibodies to newborn rats the TH level was reduced to 75% of controls after 12 h, to 48% after 24 h, 39% after 36, and 28% after 48 h. After this time no further reduction occurred and levels remained constant up to 14 days. The effect of the NGF-antibodies was reversible on addition of NGF up to 48 h after antibody administration. Although the reversibility was not complete (85% of controls) the extent of the reversibility was the same whether NGF was given 12 or 48 h after the antibodies. The incompleteness of the reversibility is reflected by the small number of degenerating neurons apparent as early as 12 h after antibody administration. Since these early degenerative effects were also seen in complement-deficient mice it is concluded that they involve a small population of neurons, sensitive to short-term NGF deprivation whereas the majority of the neurons can withstand deprivation for up to 48 h without sustaining irreversible damage.
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Collection:
01-internacional
Database:
MEDLINE
Main subject:
Complement C5
/
Adrenergic Fibers
/
Cytotoxicity, Immunologic
Limits:
Animals
Language:
En
Journal:
Brain Res
Year:
1980
Document type:
Article
Country of publication:
Netherlands